Asadollahi Reza, Zweier Markus, Gogoll Laura, Schiffmann Raphael, Sticht Heinrich, Steindl Katharina, Rauch Anita
Institute of Medical Genetics, University of Zurich, Schlieren-Zurich, Switzerland.
Institute of Metabolic Disease, Baylor Scott & White Research Institute, Dallas, TX, USA.
Eur J Med Genet. 2017 Sep;60(9):451-464. doi: 10.1016/j.ejmg.2017.06.004. Epub 2017 Jun 21.
A decade after the designation of MED13L as a gene and its link to intellectual disability (ID) and dextro-looped transposition of great arteries in 2003, we previously described a recognizable syndrome due to MED13L haploinsufficiency. Subsequent reports of 22 further patients diagnosed by genome-wide testing further delineated the syndrome with expansion of the phenotypic spectrum and showed reduced penetrance for congenital heart defects. We now report two novel patients identified by whole exome sequencing, one with a de novo MED13L truncating mutation and the other with a de novo missense mutation. The first patient indicates some facial resemblance to Kleefstra syndrome as a novel differential diagnosis, and the second patient shows, for the first time, recurrence of a MED13L missense mutation (p.(Asp860Gly)). Notably, our in silico modelling predicted this missense mutation to decrease the stability of an alpha-helix and thereby affecting the MED13L secondary structure, while the majority of published missense mutations remain variants of uncertain significance. Review of the reported patients with MED13L haploinsufficiency indicates moderate to severe ID and facial anomalies in all patients, as well as severe speech delay and muscular hypotonia in the majority. Further common signs include abnormal MRI findings of myelination defects and abnormal corpus callosum, ataxia and coordination problems, autistic features, seizures/abnormal EEG, or congenital heart defects, present in about 20-50% of the patients. With reference to facial anomalies, the majority of patients were reported to show broad/prominent forehead, low set ears, bitemporal narrowing, upslanting palpebral fissures, depressed/flat nasal bridge, bulbous nose, and abnormal chin, but macroglossia and horizontal eyebrows were also observed in ∼30%. The latter are especially important in the differential diagnosis of 1p36 deletion and Kleefstra syndromes, while the more common facial gestalt shows some resemblance to 22q11.2 deletion syndrome. Despite the fact that MED13L was found to be one of the most common ID genes in the Deciphering Developmental Disorders Study, further detailed patient descriptions are needed to explore the full clinical spectrum, potential genotype-phenotype correlations, as well as the role of missense mutations and potential mutational hotspots along the gene.
2003年MED13L被确定为一个基因并与智力残疾(ID)和大动脉右旋袢转位相关联,十年后,我们之前描述了一种由MED13L单倍体不足引起的可识别综合征。随后通过全基因组检测诊断出另外22例患者的报告进一步明确了该综合征,其表型谱有所扩展,并显示出先天性心脏缺陷的外显率降低。我们现在报告通过全外显子测序鉴定出的2例新患者,1例携带从头发生的MED13L截短突变,另1例携带从头发生的错义突变。首例患者表现出与克莱夫斯特拉综合征有一些面部相似之处,可作为一种新的鉴别诊断,第二例患者首次出现MED13L错义突变(p.(Asp860Gly))的复发。值得注意的是,我们的计算机模拟预测该错义突变会降低α-螺旋的稳定性,从而影响MED13L的二级结构,而大多数已发表的错义突变仍为意义未明的变异。对已报告的MED13L单倍体不足患者的回顾表明,所有患者均有中度至重度ID和面部异常,大多数患者还有严重的语言发育迟缓及肌张力减退。其他常见体征包括髓鞘形成缺陷和胼胝体异常的MRI表现、共济失调和协调问题、自闭症特征、癫痫发作/脑电图异常,或先天性心脏缺陷,约20% - 50%的患者有这些表现。关于面部异常,大多数患者报告有宽/突出的额头、低位耳、颞部变窄、睑裂上斜、鼻梁凹陷/扁平、球状鼻和异常下巴,但约30%的患者也观察到巨舌和水平眉。后者在1p36缺失和克莱夫斯特拉综合征的鉴别诊断中尤为重要,而更常见的面部形态与22q11.2缺失综合征有一些相似之处。尽管在“解读发育障碍研究”中发现MED13L是最常见的ID基因之一,但仍需要更详细的患者描述来探索完整的临床谱、潜在的基因型-表型相关性,以及错义突变的作用和该基因上潜在的突变热点。
